Basal-cell carcinoma

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Basal-cell carcinoma
Other names: Basal-cell skin cancer, basal cell epithelioma, basalioma[1]
Ulcerated basal-cell carcinoma affecting the skin of the nose in an elderly individual
SpecialtyDermatology, oncology
SymptomsPainless raised area of skin that may be shiny with small blood vessel running over it or ulceration, rolled edge[2]
Usual onsetAdults
TypesNodular, cystic, morpheaform, others[1]
Risk factorsLight skin, ultraviolet light, radiation therapy, arsenic, poor immune function[1]
Diagnostic methodBy its appearance, skin biopsy[2]
Differential diagnosisTrichoepithelioma,[1] squamous cell carcinoma, seborrheic keratosis, melanoma, psoriasis, sebaceous hyperplasia[2]
TreatmentSurgical removal, photodynamic therapy, radiation treatment[2]
PrognosisDepends on type, mostly good, may recur[1]
Frequency~30% of white people at some point (US)[3] males>females[1]
DeathsRare[1]

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Basal-cell carcinoma (BCC), also known as basal-cell cancer, is a type of skin cancer.[1] The classic appearance is a painless small raised bump in the skin, which may be shiny with overlying small blood vessels, and have a central dip or ulcer, crusting, or blood.[2] Larger ones may have a rolled edge.[2] Other patterns may include blue-grey fluid-filled small bumps, white plaques, or dry scaly marks.[2] There are generally no symptoms; though if scratched, they may bleed.[2] It tends to grow slowly, damage surrounding tissue, but is unlikely to spread to distant areas or result in death.[4]

Risk factors include exposure to ultraviolet light, having lighter skin, radiation therapy, long-term exposure to arsenic and poor immune-system function.[1] The use of tanning beds and exposure to UV light during childhood is particularly harmful.[1] It is believed to originate from a type of cell associated with the hair follicle.[1] Diagnosis is by its appearance and confirmed by tissue biopsy.[2]

It remains unclear whether sunscreen affects the risk of basal-cell cancer.[2] Treatment is typically by surgical removal.[2] This can be by simple excision if the cancer is small; otherwise, Mohs surgery is generally recommended.[3] Other options include electrodesiccation and curettage, cryosurgery, topical chemotherapy, photodynamic therapy, laser surgery or the use of imiquimod, a topical immune-activating medication.[5] In the rare cases in which distant spread has occurred, chemotherapy or targeted therapy may be used.[5]

Basal-cell cancer is the most common type of skin cancer and the most common cancer overall.[1] It accounts for at least 32% of all cancers globally.[6][7] Of skin cancers other than melanoma, about 80% are basal-cell cancers.[3] It occurs most frequently in Australia, where 50% of people develop BCC before the age of 70.[1] In the United States, about 35% of white males and 25% of white females are affected by BCC at some point in their lives.[3]

Signs and symptoms

Individuals with a basal-cell carcinoma typically present with a shiny, pearly skin nodule. However, superficial basal-cell cancer can present as a red patch similar to eczema. Infiltrative or morpheaform basal-cell cancers can present as a skin thickening or scar tissue – making diagnosis difficult without using tactile sensation and a skin biopsy. It is often difficult to visually distinguish basal-cell cancer from acne scar, actinic elastosis, and recent cryodestruction inflammation.[citation needed]

Cause

The majority of basal-cell carcinomas occur on sun-exposed areas of the body.[8]

Pathophysiology

Micrograph of a basal-cell carcinoma, showing the characteristic histomorphologic features (peripheral palisading, myxoid stroma, artefactual clefting). H&E stain

Basal-cell carcinomas are currently considered to have origin from the folliculo-sebaceous-apocrine germ, also known as trichoblast. The differential diagnosis with trichoblastic carcinoma, a rare malignant form of trichoblastoma, can be challenging.[9] Alternatively, one argument is that basal-cell carcinoma is trichoblastic carcinoma.[10] Overexposure to sun leads to the formation of thymine dimers, a form of DNA damage. While DNA repair removes most UV-induced damage, not all crosslinks are excised. There is, therefore, cumulative DNA damage leading to mutations. Apart from the mutagenesis, overexposure to sunlight depresses the local immune system, possibly decreasing immune surveillance for new tumor cells.

Basal-cell carcinomas can often come in association with other lesions of the skin, such as actinic keratosis, seborrheic keratosis, squamous cell carcinoma.[11] In a small proportion of cases, basal-cell carcinoma also develops as a result of basal-cell nevus syndrome, or Gorlin Syndrome, which is also characterized by keratocystic odontogenic tumors of the jaw, palmar or plantar (sole of the foot) pits, calcification of the falx cerebri (in the center line of the brain) and rib abnormalities. The cause of this syndrome is a mutation in the PTCH1 tumor suppressor gene located in chromosome 9q22.3, which inhibits the hedgehog signaling pathway. A mutation in the SMO gene, which is also on the hedgehog pathway, also causes basal-cell carcinoma.[12]

Diagnosis

To diagnose basal-cell carcinomas, a skin biopsy is performed for histopathologic analyses. The most common method is a shave biopsy under local anesthesia. Most nodular basal-cell cancers can be diagnosed clinically; however, other variants can be very difficult to distinguish from benign lesions such as intradermal naevus, sebaceomas, fibrous papules, early acne scars, and hypertrophic scarring.[13] Exfoliative cytology methods have high sensitivity and specificity for confirming the diagnosis of basal cell carcinoma when clinical suspicion is high but unclear usefulness otherwise.[14]

Characteristics

High-magnification micrograph of basal-cell carcinoma.

Basal-cell carcinoma cells appear similar to epidermal basal cells, and are usually well differentiated.[15]

In uncertain cases, immunohistochemistry using BerEP4 can be used, having a high sensitivity and specificity in detecting only BCC cells.[16]

Main classes

Basal-cell carcinoma can broadly be divided into three groups, based on the growth patterns.

  1. Superficial basal-cell carcinoma, formerly referred to in-situ basal-cell carcinoma, is characterized by a superficial proliferation of neoplastic basal-cells. This tumor is generally responsive to topic chemotherapy, such as imiquimod, or fluorouracil.
  2. Infiltrative basal-cell carcinoma, which also encompasses morpheaform and micronodular basal-cell cancer, is more difficult to treat with conservative methods, given its tendency to penetrate into deeper layers of the skin.
  3. Nodular basal-cell carcinoma includes most of the remaining categories of basal-cell cancer. It is not unusual to encounter heterogeneous morphologic features within the same tumor.

Nodular basal-cell carcinoma

Basal-cell carcinoma with nodular pattern.

Nodular basal-cell carcinoma (also known as "classic basal-cell carcinoma") accounts for between 50% and 80% of all BCC.[2] It most commonly occurs on the sun-exposed areas of the head and neck.[2] Histopathology shows aggregates of basaloid cells with well-defined borders, showing a peripheral palisading of cells and one or more typical clefts.[17] Such clefts are caused by shrinkage of mucin during tissue fixation and staining.[18] Central necrosis with eosinophilic, granular features may be also present, as well as mucin. The heavy aggregates of mucin determine a cystic structure. Calcification may be also present, especially in long-standing lesions.[17] Mitotic activity is usually not so evident, but a high mitotic rate may be present in more aggressive lesions.[17] Adenoidal BCC can be classified as a variant of NBCC, characterized by basaloid cells with a reticulated configuration extending into the dermis.[17]

Other subtypes

Other more specific subtypes of basal-cell carcinoma include:[19][2]

Type Histopathology Other characteristics Image
Cystic basal-cell carcinoma Morphologically characterized by dome-shaped, blue-gray cystic nodules.[2]
Morpheaform basal-cell carcinoma (also known as "cicatricial basal-cell carcinoma", and "morphoeic basal-cell carcinoma") Narrow strands and nests of basaloid cells, surrounded by dense sclerotic stroma.[20] Aggressive[19]: 748 [2]
Infiltrative basal-cell carcinoma Deep infiltration.[2] Aggressive[2]
Micronodular basal-cell carcinoma Small and closely spaced nests.
Superficial basal-cell carcinoma (also known as "superficial multicentric basal-cell carcinoma") Occurs most commonly on the trunk and appears as an erythematous patch.[19]: 748 [2]
Pigmented basal-cell carcinoma exhibits increased melanization.[19]: 748 [2]: 647  About 80% of all basal-cell carcinoma in Chinese are pigmented while this subtype is uncommon in white people.[citation needed]
Rodent ulcer (also known as a "Jacob's ulcer") Nodular, with central necrosis.[19]: 748 [2] Generally a large skin lesion with central necrosis.[19]: 748 [2]
Fibroepithelioma of Pinkus Anastomosing epithelial strands in a fenestrated pattern[21] Most commonly occurs on the lower back.[19]: 748 [2]
Polypoid basal-cell carcinoma Exophytic nodules (polyp-like structures) Generally on head and neck.[2]
Pore-like basal-cell carcinoma Resembles an enlarged pore or stellate pit.[2]
Aberrant basal-cell carcinoma Absence of any apparent carcinogenic factor, and occurring in odd sites such as the scrotum, vulva, perineum, nipple, and axilla.[2]

Aggressiveness patterns

There are mainly three patterns of aggressiveness, based mainly the cohesion of cancer cells:[22]

Low-level aggressive pattern Moderately aggressive pattern Highly aggressive pattern

Differential diagnoses

Main histological differential diagnoses of basal cell carcinoma:[17]
Differential diagnosis Pathological Features Image
Hair follicles Peripheral sections may look like nests, but do not display atypia, nuclei are smaller, and serial sections will reveal the rest of the hair follicle.
Squamous-cell carcinoma of the skin Squamous-cell carcinoma of the skin is generally distinguishable by for example relatively more cytoplasm, horn cyst formation and absence of palisading and cleft formations. Yet, a high prevalence means a relatively high incidence of borderline cases, such as basal-cell carcinoma with squamous cell metaplasia (H&E stain at left in image). BerEP4 staining helps in such cases, staining only basal-cell carcinoma cells (right in image).
Trichoblastoma Absence of cleft, rudimentary hair germs, papillary mesenchymal bodies.
Adenoid cystic carcinoma Lack of basaloid cells disposed in peripheral palisades; adenoid-cystic lesion without connection to the epidermis; absence of artefactual clefts
Microcystic adnexal carcinoma Bland keratinocytes, keratin cysts, ductal differentiation. BerEp4- (in 60% of cases),[24] CEA+, EMA+
Trichoepithelioma[notes 1] Rims of collagen bundles, calcification, follicular/sebaceous/infundibular differentiation and cut artefacts. Cytokeratin (CK)20+, p75+, Pleckstrin homology-like domain family A member 1 + (PHLDA1+), common acute lymphoblastic leukemiaantigen + (CD10+) in tumor stroma, CK 6-, Ki-67- and Androgen Rceptor- (AR-)
Merkel cell carcinoma Cells arranged in a diffuse, trabecular and/or nested pattern, involving also the subcutis. Mouse Anti-Cytokeratin (CAM) 5.2+, CK20+, S100-, human leukocyte common antigen- ( LCA-), thyroid transcription factor 1- (TTF1-)

Radicality

Comparison H&E stain (left) with BerEP4 immunohistochemistry staining (right) on a pathological section having BCC with squamous cell metaplasia. Only BCC cells are stained with BerEP4.[16]

In suspected but uncertain BCC cells close to the resection margins, immunohistochemistry with BerEp4 can highlight the BCC cells.

Prevention

Basal-cell carcinoma is a common skin cancer and occurs mainly in fair-skinned patients with a family history of this cancer. Sunlight is a factor in about two-thirds of these cancers; therefore, doctors recommend sunscreens with at least SPF 30. However, a Cochrane review examining the effect of solar protection (sunscreen only) in preventing the development of basal-cell carcinoma or cutaneous squamous cell carcinoma found that there was insufficient evidence to demonstrate whether sunscreen was effective for the prevention of either of these keratinocyte-derived cancers.[25] The review did ultimately state that the certainty of these results was low, so future evidence could very well alter this conclusion. One-third occur in non-sun-exposed areas; thus, the pathogenesis is more complex than UV exposure as the cause.[8]

The use of a chemotherapeutic agent such as 5-Fluorouracil or imiquimod can prevent the development of skin cancer. It is usually recommended to individuals with extensive sun damage, history of multiple skin cancers, or rudimentary forms of cancer (i.e., solar keratosis).[26] It is often repeated every 2 to 3 years to further decrease the risk of skin cancer.[citation needed]

Treatment

The following methods are employed in the treatment of basal-cell carcinoma (BCC):

Surgery

Standard surgical excision

A weakness with standard surgical excision is a reported higher recurrence rate of basal-cell cancers of the face, especially around the eyelids,[27] nose, and facial structures.[28] There is no clear approach for treating basal-cell carcinoma around the eye.[29] A diagram on page 38 of the National Comprehensive Cancer Network publication demonstrate the area of high risk of recurrence as being most of the face with the exception of the central cheek and upper forehead.[30]

For ill-defined or recurrent basal-cell cancer on the face after previous surgery, special surgical margin controlled processing (CCPDMA – complete circumferential peripheral and deep margin assessment[30])[31] using frozen section histology (Mohs surgery is one of the methods) should be considered.[32][33] The pathologist processing the frozen section specimen should cut multiple sections through the block to minimize the false negative error rate. Or one should simply process the tissue utilizing a method approximating the Mohs method (described in most basic histopathology text books or described in this reference [32]) during frozen section processing. Unfortunately, these methods are difficult when applied to frozen sections; and they are very tedious to process. When not utilizing frozen section, the surgeon might have to wait a week or more before informing the patient if more tumour is left, or if the surgical margin is too narrow.[34] A second surgery must be performed to remove the residual or potential residual tumour once the surgeon informs the patient of the positive or narrow surgical margin on the surgical pathology report.

For poorly defined or recurrent tumours on the face, Mohs surgery or frozen section histology with either margin control (ccpdma) or thin serial bread-loafing should be considered.[30] However, most standard excisions done in a plastic surgeon or dermatologist's office are sent to an outside laboratory for standard bread loafing method of processing.[35] With this method, it is likely that less than 5% of the surgical margin is examined, as each slice of tissue is only 6 micrometres thick, about 3 to 4 serial slices are obtained per section, and only about 3 to 4 sections are obtained per specimen.[36] A meta-analysis of randomized controlled trials supports surgery as the most effective treatment of BCC of the skin.[37] There is no clear research comparing the effectiveness of Mohs micrographic surgery versus surgical excision for BCC of the eye.[29]

Mohs surgery

Mohs surgery (or Mohs micrographic surgery) is an outpatient procedure, which was developed by Frederic E. Mohs in the 1940s,[38] in which the tumor is surgically excised and then immediately examined under a microscope. It is a form of pathology processing called CCPDMA. The base and edges are microscopically examined to verify sufficient margins before the surgical repair of the site. If the margins are insufficient, more is removed from the patient until the margins are sufficient. It is also used for squamous-cell carcinoma; however, the cure rate is not as high as Mohs surgery for basal-cell carcinoma. The 2008 study found MMS to be a good option for both primary and high-risk recurrent BCCs.[38]

Cryosurgery

Cryosurgery is an old modality for the treatment of many skin cancers. When accurately utilized with a temperature probe and cryotherapy instruments, it can result in very good cure rate. Disadvantages include lack of margin control, tissue necrosis, over or under treatment of the tumor, and long recovery time. Overall, there are sufficient data to consider cryosurgery as a reasonable treatment for BCC. There are no good studies, however, comparing cryosurgery with other modalities, particularly with Mohs surgery, excision, or electrodesiccation and curettage so that no conclusion can be made whether cryosurgery is as efficacious as other methods. Also, there is no evidence on whether curetting the lesions before cryosurgery affects the efficacy of treatment.[39] Several textbooks are published on the therapy, and a few physicians still apply the treatment to selected patients.[40]

Electrodesiccation and curettage

Electrodesiccation and curettage (EDC, also known as curettage and cautery, simply curettage)[38] is accomplished by using a round knife, or curette, to scrape away the soft cancer. The skin is then burned with an electric current. This further softens the skin, allowing for the knife to cut more deeply with the next layer of curettage. The cycle is repeated, with a safety margin of curettage of normal skin around the visible tumor. This cycle is repeated 3 to 5 times, and the free skin margin treated is usually 4 to 6 mm. Cure rate is very much user-dependent and depends also on the size and type of tumor. Infiltrative or morpheaform BCCs can be difficult to eradicate with EDC. Generally, this method is used on cosmetically unimportant areas like the trunk (torso). Some physicians believe that it is acceptable to utilize EDC on the face of elderly patients over the age of 70. However, with increasing life expectancy, such an objective criterion cannot be supported. The cure rate can vary, depending on the aggressiveness of the EDC and the free margin treated. Some advocate curettage alone without electrodesiccation, and with the same cure rate.[41]

Chemotherapy

Some superficial cancers respond to local therapy with 5-fluorouracil, a chemotherapy agent. Topical treatment with 5% imiquimod cream, with five applications per week for six weeks has a reported 70–90% success rate at reducing, even removing, the BCC [basal-cell carcinoma]. Both Imiquimod and 5-fluorouracil have received FDA approval, and topical IMQ is approved by the European Medicines Agency for treatment of small superficial basal-cell carcinoma.[38] Off label use of imiquimod on invasive basal-cell carcinoma has been reported. Imiquimod may be used prior to surgery in order to reduce the size of the carcinoma. One can expect a great deal of inflammation with this treatment.[42] Chemotherapy often follows Mohs surgery to eliminate the residual superficial basal-cell carcinoma after the invasive portion is removed. Some advocate the use of imiquimod prior to Mohs surgery to remove the superficial component of the cancer.[43]

Removing the residual superficial tumor with surgery alone can result in large and difficult to repair surgical defects. One often waits a month or more after surgery before starting the Imiquimod or 5-fluorouracil to make sure the surgical wound has adequately healed. Some people[who?] advocate the use of curettage (see EDC below) first, followed by chemotherapy. These experimental procedures are not standard care.[38]

Vismodegib and sonidegib are drugs approved for specially treating BCC, but are expensive and cannot be used in pregnant women.

Immunotherapy

Immunotherapy research suggests that treatment using Euphorbia peplus, a common garden weed, may be effective.[44] Australian biopharmaceutical company Peplin[45] is developing this as topical treatment for BCC. Imiquimod is an immunotherapy but is listed here under chemotherapy.

Radiation

Radiation therapy can be delivered either as external beam radiotherapy or as brachytherapy (internal radiotherapy). Although radiotherapy is generally used in older patients who are not candidates for surgery, it is also used in cases where surgical excision will be disfiguring or difficult to reconstruct (especially on the tip of the nose, and the nostril rims). Radiation treatment often takes as few as 5 visits to as many as 25 visits. Usually, the more visits scheduled for therapy, the less complication or damage is done to the normal tissue supporting the tumor. Radiotherapy can also be useful if surgical excision has been done incompletely or if the pathology report following surgery suggests a high risk of recurrence, for example if nerve involvement has been demonstrated. Cure rate can be as high as 95% for small tumor, or as low as 80% for large tumors.

Usually, recurrent tumors after radiation are treated with surgery, and not with radiation. Further radiation treatment will further damage normal tissue, and the tumor might be resistant to further radiation. Radiation therapy may be contraindicated for treatment of nevoid basal-cell carcinoma syndrome. A meta-analysis of randomized controlled trials supports radiotherapy as one of the most effective treatments for BCC.[37] A 2008 study reported that radiation therapy is appropriate for primary BCCs and recurrent BCCs, but not for BCCs that have recurred following previous radiation treatment.[38]

Photodynamic therapy

Photodynamic therapy (PDT) is a new modality for treatment of basal-cell carcinoma, which is administrated by application of photosensitizers to the target area. When these molecules are activated by light, they become toxic, therefore destroy the target cells. Methyl aminolevulinate is approved by EU as a photosensitizer since 2001. This therapy is also used in other skin cancer types.[46] The 2008 study reported that PDT was a good treatment option for primary superficial BCCs and reasonable for primary low-risk nodular BCCs but a "relatively poor" option for high-risk lesions.[38]

Prognosis

Prognosis is excellent if the appropriate method of treatment is used in early primary basal-cell cancers. Recurrent cancers are much harder to cure, with a higher recurrent rate with any methods of treatment. Although basal-cell carcinoma rarely metastasizes, it grows locally with invasion and destruction of local tissues. The cancer can impinge on vital structures like nerves and result in loss of sensation or loss of function or rarely death. The vast majority of cases can be successfully treated before serious complications occur. The recurrence rate for the above treatment options ranges from 50 percent to 1 percent or less.

Epidemiology

Basal-cell cancer is the most common type of skin cancer and the most common cancer overall.[1] It occurs at least three times more frequently than squamous cell carcinoma in people who do not have weakened immune systems.[4] Most occur on the nose.[4] This tumor accounts for approximately 70% of non-melanoma skin cancers. In 80 percent of all cases, BCC affects the skin of head and neck, with increasing numbers affecting the trunk.[47]

It occurs most frequently in Australia, where 50% of people there will develop BCC before reaching the age of 70 years.[1] It is much more common in fair-skinned individuals with a family history of BCC and increases in incidence closer to the equator or at higher altitude. There are approximately 800,000[48] new cases yearly in the United States alone. Up to 30% of White people develop basal-cell carcinomas in their lifetime.[47] In Canada, the most common skin cancer is basal-cell carcinoma (as much as one third of all cancer diagnoses), affecting 1 in 7 individuals over a lifetime.[49]

Most sporadic BCC arises in small numbers on sun-exposed skin of people over age 50, although younger people may also be affected. The development of multiple basal-cell cancer at an early age could be indicative of nevoid basal-cell carcinoma syndrome, also known as Gorlin Syndrome.[50]

Notes

  1. Desmoplastic tricoepithelioma is particularly similar to basal-cell carcinoma.

See also

References

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